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无痕β-巯基辅助的缬氨酰苯并咪唑啉酮在肽连接中的活化作用。

Traceless β-mercaptan-assisted activation of valinyl benzimidazolinones in peptide ligations.

作者信息

Wang Yinglu, Han Lin, Yuan Ning, Wang Hanxuan, Li Hongxing, Liu Jinrong, Chen Huan, Zhang Qiang, Dong Suwei

机构信息

State Key Laboratory of Natural and Biomimetic Drugs , Department of Chemical Biology , School of Pharmaceutical Sciences , Peking University , Beijing 100191 , China . Email:

Department of Chemistry , University at Albany , Albany , New York 12222 , USA . Email:

出版信息

Chem Sci. 2018 Jan 5;9(7):1940-1946. doi: 10.1039/c7sc04148a. eCollection 2018 Feb 21.

Abstract

Peptidyl thioesters or their surrogates with C-terminal β-branched hydrophobic amino acid residues usually exhibit poor reactivities in ligation reactions. Thus, activation using exogenous additives is required to ensure an acceptable reaction efficiency. Herein, we report a traceless ligation at Val-Xaa sites under mild thiol additive-free reaction conditions, whereby the introduction of β-mercaptan on the C-terminal valine residue effectively activates the otherwise unreactive -acyl-benzimidazolinone (Nbz), and enables the use of a one-pot ligation-desulfurization strategy to generate the desired peptide products. The orthogonality between β-thiovaline-Nbz and a conventional alkyl thioester, as well as the convenient access to the former from readily available penicillamine, also allowed expedited assembly of the peptidic hormone β-LPH and hPTH analogues, based on a kinetically controlled one-pot three-segment ligation and desulfurization strategy.

摘要

具有C端β-支链疏水氨基酸残基的肽基硫酯或其替代物通常在连接反应中表现出较差的反应活性。因此,需要使用外源添加剂进行活化以确保可接受的反应效率。在此,我们报道了在无硫醇添加剂的温和反应条件下在Val-Xaa位点进行无痕连接,由此在C端缬氨酸残基上引入β-巯基有效地活化了原本无反应性的-酰基-苯并咪唑啉酮(Nbz),并使得能够使用一锅法连接-脱硫策略来生成所需的肽产物。β-硫代缬氨酸-Nbz与传统烷基硫酯之间的正交性,以及从易得的青霉胺方便地获得前者,还基于动力学控制的一锅三段连接和脱硫策略实现了肽激素β-LPH和hPTH类似物的快速组装。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1998/5892131/4836913cefbd/c7sc04148a-f1.jpg

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